Factors associated with HPV-DNA clearance in a cohort of HIV-positive patients: role of cART and gender

2014 
Introduction: We aimed to assess any factors associated with dysplasia regression and with HPV clearance in a cohort of HIV patients, with particular focus on cART and gender. Methods: Asymptomatic HIV patients of the San Paolo Infectious Disease (SPID) cohort who underwent anoscopy/ gynaecological evaluation were enrolled. Anal/cervical brushing were analyzed for: HPV-PCR detection/genotyping (HR-HPV), cytologic abnormalities (Bethesda System 2001: LSIL-HSIL). Demographics and HIV-related parameters were evaluated at baseline. Activated CD8 /CD38 lymphocytes were measured (flow citometry). Patients were examined at baseline (T0) and at 12 18 months visit (T1). HPV clearance was defined as negativisation of HPV at T1; SIL regression (SIL-R) and progression (SILP) were defined as change from HSIL/LSIL to a lower-grade/absence of dysplasia and as change from absence of HSIL/LSIL to a higher-grade dysplasia at T1, respectively. Mann Whitney test, Chi-square test and multivariate logistic regression were used. Results: A total of 189 patients were examined, 60 (32%) were women. One hundred fifty patients (79%) were HPV , 113 (75%) harboured HR-HPV; 103 (68%) showed LSIL/HSIL at T0 (32% of women and 65% of men) (all were HPV-positive). No differences in demographics and HIV-related markers were found between patients with SIL-P (33, 41%) and patients with SIL-R (47, 59%). HPV patients who cleared HPV (28, 18%) were found to be more frequently female, heterosexual infected, more frequently on cART and with lower Log10 HIV-RNA and lower levels of CD8 /CD38 % compared with HPV persistence group (Table 1). No differences in PI exposure were found between the two groups (p .08). Interestingly, also when only HR-HPV were considered, clearance was associated with exposure to cART (naive 4%, vs cART 86%, p .048). In multivariate analysis, heterosexuals (AOR 5.123, 95% CI 1.5 17.5 vs homosexuals) were independently associated to HPV clearance, whereas CD8 / CD38 % (AOR 0.44, 95% CI 0.65 1.01 for each % more) were predictive of HPV persistence. Conclusions: Close follow-up of HPV and SIL should be promoted particularly in men and in untreated individuals. We cannot exclude behavioural variables linked to risky sex and reinfection.
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